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Monitoring the dynamics of Src activity in response to anti-invasive dasatinib treatment at a subcellular level using dual intravital imaging

机译:使用双重活体成像技术在亚细胞水平上监测响应抗侵入性达沙替尼治疗的Src活性动态

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摘要

Optimising response to tyrosine kinase inhibitors in cancer remains an extensive field of research. Intravital imaging is an emerging tool, which can be used in drug discovery to facilitate and fine-tune maximum drug response in live tumors. A greater understanding of intratumoural delivery and pharmacodynamics of a drug can be obtained by imaging drug target-specific fluorescence resonance energy transfer (FRET) biosensors in real time. Here, we outline our recent work using a Src-FRET biosensor as a readout of Src activity to gauge optimal tyrosine kinase inhibition in response to dasatinib treatment regimens in vivo. By simultaneously monitoring both the inhibition of Src using FRET imaging, and the modulation of the surrounding extracellular matrix using second harmonic generation (SHG) imaging, we were able to show enhanced drug penetrance and delivery to live pancreatic tumors. We discuss the implications of this dual intravital imaging approach in the context of altered tumor-stromal interactions, while summarising how this approach could be applied to assess other combination strategies or tyrosine kinase inhibitors in a preclinical setting.
机译:在癌症中优化对酪氨酸激酶抑制剂的反应仍是广泛的研究领域。活体成像是一种新兴工具,可用于药物发现,以促进和调整活体肿瘤中的最大药物反应。通过实时对药物靶标特异性荧光共振能量转移(FRET)生物传感器进行成像,可以更好地了解药物在肿瘤内的传递和药效。在这里,我们概述了我们最近使用Src-FRET生物传感器作为Src活性的读数来测量对达沙替尼治疗方案体内的最佳酪氨酸激酶抑制的反应。通过同时监测使用FRET成像对Src的抑制和使用二次谐波生成(SHG)成像对周围细胞外基质的调节,我们能够显示出增强的药物渗透性和向活体胰腺肿瘤的递送。我们讨论了这种双重活体成像方法在改变的肿瘤间质相互作用中的意义,同时总结了该方法如何可用于在临床前环境中评估其他联合策略或酪氨酸激酶抑制剂。

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